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Lead selection and characterization of antitubercular compounds using the Nested Chemical Library

Authors :
Natassja G. Bush
László Őrfi
Ruben C. Hartkoorn
László Kékesi
Adwait Anand Godbole
Katarína Mikušová
György Kéri
Anthony Maxwell
Zuzana Svetlíková
János Pató
Stewart T. Cole
Csaba Szántai-Kis
Valakunja Nagaraja
Anna Sipos
Jana Korduláková
Rita Székely
Frédéric Collin
Source :
IndraStra Global.
Publication Year :
2015
Publisher :
CHURCHILL LIVINGSTONE, 2015.

Abstract

Discovering new drugs to treat tuberculosis more efficiently and to overcome multidrug resistance is a world health priority. To find novel antitubercular agents several approaches have been used in various institutions worldwide, including target-based approaches against several validated mycobacterial enzymes and phenotypic screens. We screened more than 17,000 compounds from Vichem's Nested Chemical Library(TM) using an integrated strategy involving whole cell-based assays with Corynebacterium glutamicum and Mycobacterium tuberculosis, and target-based assays with protein kinases PknA, PknB and PknG as well as other targets such as PimA and bacterial topoisomerases simultaneously. With the help of the target-based approach we have found very potent hits inhibiting the selected target enzymes, but good minimal inhibitory concentrations (MIC) against M. tuberculosis were not achieved. Focussing on the whole cell-based approach several potent hits were found which displayed minimal inhibitory concentrations (MIC) against M. tuberculosis below 10 mu M and were non-mutagenic, non-cytotoxic and the targets of some of the hits were also identified. The most active hits represented various scaffolds. Medicinal chemistry-based lead optimization was performed applying various strategies and, as a consequence, a series of novel potent compounds were synthesized. These efforts resulted in some effective potential antitubercular lead compounds which were confirmed in phenotypic assays. (C) 2015 Elsevier Ltd. All rights reserved.

Details

Language :
English
ISSN :
23813652
Database :
OpenAIRE
Journal :
IndraStra Global
Accession number :
edsair.doi.dedup.....1fff1f81b2dcba388155a20b6edf4779